A diverse family of novel peptide toxins from an unusual cone snail, Conus californicus

Author:

Gilly W. F.1,Richmond T. A.2,Duda T. F.3,Elliger C.1,Lebaric Z.1,Schulz J.4,Bingham J. P.5,Sweedler J. V.6

Affiliation:

1. Hopkins Marine Station, Stanford University, Pacific Grove, CA 93950, USA

2. Department of Chemistry, Tabor College, Hillsboro, KS 67063, USA

3. Department of Ecology and Evolutionary Biology and Museum of Zoology, University of Michigan, Ann Arbor, MI 48109, USA and Smithsonian Tropical Research Institute, Balboa, Panama

4. Department of Biology, Occidental College, Los Angeles, CA 90041USA

5. Department of Molecular Biosciences and Bioengineering, University of Hawaii, Honolulu, HI 96822, USA

6. Department of Chemistry, University of Illinois, Urbana, IL 61801, USA

Abstract

SUMMARY Diversity among Conus toxins mirrors the high species diversity in the Indo-Pacific region, and evolution of both is thought to stem from feeding-niche specialization derived from intra-generic competition. This study focuses on Conus californicus, a phylogenetic outlier endemic to the temperate northeast Pacific. Essentially free of congeneric competitors, it preys on a wider variety of organisms than any other cone snail. Using molecular cloning of cDNAs and mass spectrometry, we examined peptides isolated from venom ducts to elucidate the sequences and post-translational modifications of two eight-cysteine toxins (cal12a and cal12b of type 12 framework) that block voltage-gated Na+ channels. Based on homology of leader sequence and mode of action, these toxins are related to the O-superfamily, but differ significantly from other members of that group. Six of the eight cysteine residues constitute the canonical framework of O-members, but two additional cysteine residues in the N-terminal region define an O+2 classification within the O-superfamily. Fifteen putative variants of Cal12.1 toxins have been identified by mRNAs that differ primarily in two short hypervariable regions and have been grouped into three subtypes (Cal12.1.1–3). This unique modular variation has not been described for other Conus toxins and suggests recombination as a diversity-generating mechanism. We propose that these toxin isoforms show specificity for similar molecular targets (Na+ channels) in the many species preyed on by C. californicus and that individualistic utilization of specific toxin isoforms may involve control of gene expression.

Publisher

The Company of Biologists

Subject

Insect Science,Molecular Biology,Animal Science and Zoology,Aquatic Science,Physiology,Ecology, Evolution, Behavior and Systematics

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